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Hair Follicle Dermal Sheath Derived Cells Improve Islet Allograft Survival without Systemic Immunosuppression

Immunosuppressive drugs successfully prevent rejection of islet allografts in the treatment of type I diabetes. However, the drugs also suppress systemic immunity increasing the risk of opportunistic infection and cancer development in allograft recipients. In this study, we investigated a new treat...

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Autores principales: Wang, Xiaojie, Hao, Jianqiang, Leung, Gigi, Breitkopf, Trisia, Wang, Eddy, Kwong, Nicole, Akhoundsadegh, Noushin, Warnock, Garth L., Shapiro, Jerry, McElwee, Kevin J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi Publishing Corporation 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4427120/
https://www.ncbi.nlm.nih.gov/pubmed/26000314
http://dx.doi.org/10.1155/2015/607328
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author Wang, Xiaojie
Hao, Jianqiang
Leung, Gigi
Breitkopf, Trisia
Wang, Eddy
Kwong, Nicole
Akhoundsadegh, Noushin
Warnock, Garth L.
Shapiro, Jerry
McElwee, Kevin J.
author_facet Wang, Xiaojie
Hao, Jianqiang
Leung, Gigi
Breitkopf, Trisia
Wang, Eddy
Kwong, Nicole
Akhoundsadegh, Noushin
Warnock, Garth L.
Shapiro, Jerry
McElwee, Kevin J.
author_sort Wang, Xiaojie
collection PubMed
description Immunosuppressive drugs successfully prevent rejection of islet allografts in the treatment of type I diabetes. However, the drugs also suppress systemic immunity increasing the risk of opportunistic infection and cancer development in allograft recipients. In this study, we investigated a new treatment for autoimmune diabetes using naturally immune privileged, hair follicle derived, autologous cells to provide localized immune protection of islet allotransplants. Islets from Balb/c mouse donors were cotransplanted with syngeneic hair follicle dermal sheath cup cells (DSCC, group 1) or fibroblasts (FB, group 2) under the kidney capsule of immune-competent, streptozotocin induced, diabetic C57BL/6 recipients. Group 1 allografts survived significantly longer than group 2 (32.2 ± 12.2 versus 14.1 ± 3.3 days, P < 0.001) without administration of any systemic immunosuppressive agents. DSCC reduced T cell activation in the renal lymph node, prevented graft infiltrates, modulated inflammatory chemokine and cytokine profiles, and preserved better beta cell function in the islet allografts, but no systemic immunosuppression was observed. In summary, DSCC prolong islet allograft survival without systemic immunosuppression by local modulation of alloimmune responses, enhancing of beta cell survival, and promoting of graft revascularization. This novel finding demonstrates the capacity of easily accessible hair follicle cells to be used as local immunosuppression agents in islet transplantation.
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spelling pubmed-44271202015-05-21 Hair Follicle Dermal Sheath Derived Cells Improve Islet Allograft Survival without Systemic Immunosuppression Wang, Xiaojie Hao, Jianqiang Leung, Gigi Breitkopf, Trisia Wang, Eddy Kwong, Nicole Akhoundsadegh, Noushin Warnock, Garth L. Shapiro, Jerry McElwee, Kevin J. J Immunol Res Research Article Immunosuppressive drugs successfully prevent rejection of islet allografts in the treatment of type I diabetes. However, the drugs also suppress systemic immunity increasing the risk of opportunistic infection and cancer development in allograft recipients. In this study, we investigated a new treatment for autoimmune diabetes using naturally immune privileged, hair follicle derived, autologous cells to provide localized immune protection of islet allotransplants. Islets from Balb/c mouse donors were cotransplanted with syngeneic hair follicle dermal sheath cup cells (DSCC, group 1) or fibroblasts (FB, group 2) under the kidney capsule of immune-competent, streptozotocin induced, diabetic C57BL/6 recipients. Group 1 allografts survived significantly longer than group 2 (32.2 ± 12.2 versus 14.1 ± 3.3 days, P < 0.001) without administration of any systemic immunosuppressive agents. DSCC reduced T cell activation in the renal lymph node, prevented graft infiltrates, modulated inflammatory chemokine and cytokine profiles, and preserved better beta cell function in the islet allografts, but no systemic immunosuppression was observed. In summary, DSCC prolong islet allograft survival without systemic immunosuppression by local modulation of alloimmune responses, enhancing of beta cell survival, and promoting of graft revascularization. This novel finding demonstrates the capacity of easily accessible hair follicle cells to be used as local immunosuppression agents in islet transplantation. Hindawi Publishing Corporation 2015 2015-04-27 /pmc/articles/PMC4427120/ /pubmed/26000314 http://dx.doi.org/10.1155/2015/607328 Text en Copyright © 2015 Xiaojie Wang et al. https://creativecommons.org/licenses/by/3.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Wang, Xiaojie
Hao, Jianqiang
Leung, Gigi
Breitkopf, Trisia
Wang, Eddy
Kwong, Nicole
Akhoundsadegh, Noushin
Warnock, Garth L.
Shapiro, Jerry
McElwee, Kevin J.
Hair Follicle Dermal Sheath Derived Cells Improve Islet Allograft Survival without Systemic Immunosuppression
title Hair Follicle Dermal Sheath Derived Cells Improve Islet Allograft Survival without Systemic Immunosuppression
title_full Hair Follicle Dermal Sheath Derived Cells Improve Islet Allograft Survival without Systemic Immunosuppression
title_fullStr Hair Follicle Dermal Sheath Derived Cells Improve Islet Allograft Survival without Systemic Immunosuppression
title_full_unstemmed Hair Follicle Dermal Sheath Derived Cells Improve Islet Allograft Survival without Systemic Immunosuppression
title_short Hair Follicle Dermal Sheath Derived Cells Improve Islet Allograft Survival without Systemic Immunosuppression
title_sort hair follicle dermal sheath derived cells improve islet allograft survival without systemic immunosuppression
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4427120/
https://www.ncbi.nlm.nih.gov/pubmed/26000314
http://dx.doi.org/10.1155/2015/607328
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